bims-agimec Biomed News
on Aging mechanisms
Issue of 2024‒07‒28
seven papers selected by
Metin Sökmen, Ankara Üniversitesi
  1. Pivotal role of AGE-RAGE axis in brain aging with current interventions.
  2. Achilles' spear: A new therapeutic target for age-related diseases.
  3. LINE-1 transposable element renaissance in aging and age-related diseases.
  4. Nur77 improves ovarian function in reproductive aging mice by activating mitophagy and inhibiting apoptosis.
  5. Autophagy in aging-related diseases and cancer: Principles, regulatory mechanisms and therapeutic potential.
  6. Biological resilience in health and disease.
  7. The association of metabolic syndrome with telomere length as a marker of cellular aging: a systematic review and meta-analysis.
  1. Ageing Res Rev. 2024 Jul 18. pii: S1568-1637(24)00247-2. [Epub ahead of print]100 102429
    Pivotal role of AGE-RAGE axis in brain aging with current interventions.
    Nikolaos Vitorakis, Christina Piperi.
      Brain aging is characterized by several structural, biochemical and molecular changes which can vary among different individuals and can be influenced by genetic, environmental and lifestyle factors. Accumulation of protein aggregates, altered neurotransmitter composition, low-grade chronic inflammation and prolonged oxidative stress have been shown to contribute to brain tissue damage. Among key metabolic byproducts, advanced glycation end products (AGEs), formed endogenously through non-enzymatic reactions or acquired directly from the diet or other exogenous sources, have been detected to accumulate in brain tissue, exerting detrimental effects on cellular structure and function, contributing to neurodegeneration and cognitive decline. Upon binding to signal transduction receptor RAGE, AGEs can initiate pro-inflammatory pathways, exacerbate oxidative stress and neuroinflammation, thus impairing neuronal function and cognition. AGE-RAGE signaling induces programmed cell death, disrupts the blood-brain barrier and promotes protein aggregation, further compromising brain health. In this review, we investigate the intricate relationship between the AGE-RAGE pathway and brain aging in order to detect affected molecules and potential targets for intervention. Reduction of AGE deposition in brain tissue either through novel pharmacological therapeutics, dietary modifications, and lifestyle changes, shows a great promise in mitigating cognitive decline associated with brain aging.
    Keywords:  AGE; Brain aging; Inflammation; Oxidative stress; RAGE
    DOI:  https://doi.org/10.1016/j.arr.2024.102429
  2. Aging Cell. 2024 Jul;23(7): e14257
    Achilles' spear: A new therapeutic target for age-related diseases.
    Yang Xuan, Yue Duan.
      The role of the senescence-associated secretory phenotype (SASP) in the development of age-related diseases is significant, and its control promises to have a tremendous positive impact on health. A recent study has identified a new mechanism for SASP regulation, titled miMOMP. Failure to regulate SASP would dramatically increase the risk of various age-related health problems. Nonetheless, we have not completely comprehended how to modulate SASP. In this commentary, we summarise the specific mechanisms by which miMOMP regulates SASP and outline possible future research directions. Moreover, potential risks and obstacles to the clinical translation of miMOMP are also presented.
    Keywords:  SASP; age‐related diseases; miMOMP; mtDNA
    DOI:  https://doi.org/10.1111/acel.14257
  3. Ageing Res Rev. 2024 Jul 24. pii: S1568-1637(24)00258-7. [Epub ahead of print] 102440
    LINE-1 transposable element renaissance in aging and age-related diseases.
    Xiang Li, Huaxin Yu, Dong Li, Na Liu.
      Transposable elements (TEs) are essential components of eukaryotic genomes and are subject to stringent regulatory mechanisms to avoid their potentially deleterious effects. However, numerous studies have verified the resurrection of TEs, particularly long interspersed nuclear element-1 (LINE-1), during preimplantation development, aging, cancer, and other age-related diseases. The LINE-1 family has also been implicated in several aging-related processes, including genomic instability, loss of heterochromatin, DNA methylation, and the senescence-associated secretory phenotype (SASP). Additionally, the role of the LINE-1 family in cancer development has also been substantiated. Research in this field has offered valuable insights into the functional mechanisms underlying LINE-1 activity, enhancing our understanding of aging regulation. This review provides a comprehensive summary of current findings on LINE-1 and their roles in aging and age-related diseases.
    Keywords:  LINE-1; aging; epigenetics; transposable elements
    DOI:  https://doi.org/10.1016/j.arr.2024.102440
  4. Reprod Biol Endocrinol. 2024 Jul 23. 22(1): 86
    Nur77 improves ovarian function in reproductive aging mice by activating mitophagy and inhibiting apoptosis.
    Ying Yao, Bin Wang, Kaihua Yu, Ji Song, Liyan Wang, Xuehong Zhang, Yulan Li.
      Reproductive aging not only affects the fertility and physical and mental health of women but also accelerates the aging process of other organs. There is an urgent need newfor novel mechanisms, targets, and drugs to break the vicious cycle of mitochondrial dysfunction, redox imbalance, and germ cell apoptosis associated with ovarian aging. Autophagy, recognized as a longevity mechanism, has recently become a focal point in anti-aging research. Although mitophagy is a type of autophagy, its role and regulatory mechanisms in ovarian aging, particularly in age-related ovarian function decline, remain unclear. Nerve growth factor inducible gene B (Nur77) is an early response gene that can be stimulated by oxidative stress, DNA damage, metabolism, and inflammation. Recent evidence recommends that decreased expression of Nur77 is associated with age-related myocardial fibrosis, renal dysfunction, and Parkinson's disease; however, its association with ovarian aging has not been studied yet. We herein identified Nur77 as a regulator of germ cell senescence, apoptosis, and mitophagy and found that overexpression of Nur77 can activate mitophagy, improve oxidative stress, reduce apoptosis, and ultimately enhance ovarian reserve in aged mice ovaries. Furthermore, we discovered an association between Nur77 and the AKT pathway through String and molecular docking analyses. Experimental confirmation revealed that the AKT/mTOR signaling pathway is involved in the regulation of Nur77 in ovarian function. In conclusion, our results suggest Nur77 as a promising target for preventing and treating ovarian function decline related to reproductive aging.
    Keywords:  Aging; Apoptosis; Granulosa cells; Mitophagy; Nur77; PINK1/Parkin
    DOI:  https://doi.org/10.1186/s12958-024-01250-6
  5. Ageing Res Rev. 2024 Jul 20. pii: S1568-1637(24)00246-0. [Epub ahead of print] 102428
    Autophagy in aging-related diseases and cancer: Principles, regulatory mechanisms and therapeutic potential.
    Na Wu, Wenhui Zheng, Yundong Zhou, Yu Tian, Min Tang, Xiaoqiang Feng, Milad Ashrafizadeh, Yuzhuo Wang, Xiaojia Niu, Murtaza Tambuwala, Lingzhi Wang, Vinay Tergaonkar, Gautam Sethi, Daniel Klionsky, Li Huang, Ming Gu.
      Macroautophagy/autophagy is primarily accountable for the degradation of damaged organelles and toxic macromolecules in the cells. Regarding the essential function of autophagy for preserving cellular homeostasis, changes in, or dysfunction of, autophagy flux can lead to disease development. In the current paper, the complicated function of autophagy in aging-associated pathologies and cancer is evaluated, highlighting the underlying molecular mechanisms that can affect longevity and disease pathogenesis. As a natural biological process, a reduction in autophagy is observed with aging, resulting in an accumulation of cell damage and the development of different diseases, including neurological disorders, cardiovascular diseases, and cancer. The MTOR, AMPK, and ATG proteins demonstrate changes during aging, and they are promising therapeutic targets. Insulin/IGF1, TOR, PKA, AKT/PKB, caloric restriction and mitochondrial respiration are vital for lifespan regulation and can modulate or have an interaction with autophagy. The specific types of autophagy, such as mitophagy that degrades mitochondria, can regulate aging by affecting these organelles and eliminating those mitochondria with genomic mutations. Autophagy and its specific types contribute to the regulation of carcinogenesis and they are able to dually enhance or decrease cancer progression. Cancer hallmarks, including proliferation, metastasis, therapy resistance and immune reactions, are tightly regulated by autophagy, supporting the conclusion that autophagy is a promising target in cancer therapy.
    Keywords:  Aging; autophagy; cancer therapy; cell death; longevity
    DOI:  https://doi.org/10.1016/j.arr.2024.102428
  6. Dis Model Mech. 2024 Jul 01. pii: dmm050799. [Epub ahead of print]17(7):
    Biological resilience in health and disease.
    Helen Weavers.
      All living organisms - from single-celled prokaryotes through to invertebrates and humans - are frequently exposed to numerous challenges during their lifetime, which could damage their molecular and cellular contents and threaten their survival. Nevertheless, these diverse organisms are, on the whole, remarkably resilient to potential threats. Recent years have seen rapid advances in our mechanistic understanding of this emerging phenomenon of biological resilience, which enables cells, tissues and whole organisms to bounce back from challenges or stress. In this At a Glance article, I discuss current knowledge on the diverse molecular mechanisms driving biological resilience across scales, with particular focus on its dynamic and adaptive nature. I highlight emerging evidence that loss of biological resilience could underly numerous pathologies, including age-related frailty and degenerative disease. Finally, I present the multi-disciplinary experimental approaches that are helping to unravel the causal mechanisms of resilience and how this emerging knowledge could be harnessed therapeutically in the clinic.
    Keywords:  Antimicrobial resistance; Cell survival; Cytoprotection; Degenerative disease; Healthy ageing; Hormesis; Stress adaptation; Tumour adaptation
    DOI:  https://doi.org/10.1242/dmm.050799
  7. Front Genet. 2024 ;15 1390198
    The association of metabolic syndrome with telomere length as a marker of cellular aging: a systematic review and meta-analysis.
    Sulieman Ibraheem Shelash Al-Hawary, Abdullah Ali Alzahrani, Hatem Ghaleb Maabreh, Mohammed Abed Jawad, Salim B Alsaadi, Noura Kareem Jabber, Ahmed Alawadi, Ali Alsalamy, Farideh Alizadeh.
      Background: It has been suggested that metabolic syndrome (MetS) accelerates the aging process, potentially contributing to the development of age-related complications. Available studies examining the relation of MetS to telomere length (TL), a putative biological marker of aging, have yielded inconclusive findings. This meta-analysis was performed to investigate the association between MetS and TL.Methods: A comprehensive systematic search was conducted in PubMed and Scopus databases to identify relevant literature published up to February 2024. Standard mean difference (SMD) and standardized beta coefficient (β) with their 95% confidence intervals (CI) were used as effect sizes to measure the associations using the random effects model.
    Results: A total of nine studies, comprising a total sample size of 8,606 participants, were eligible for the meta-analysis. No significant difference in mean TL was found between patients with and without MetS (SMD = -0.03, 95%CI = -0.17 to 0.10), with a significant heterogeneity across the studies (I 2 = 89.7.0%, p ≤ 0.001). In contrast, it was revealed that MetS is negatively related to TL (β = -0.08, 95%CI = -0.15 to -0.004). In the subgroup analysis, this finding was supported by the International Diabetes Federation (IDF) definition of MetS.
    Conclusion: This meta-analysis highlighted that MetS may be linked to a shorter TL. Additional studies are required to confirm this finding.
    Keywords:  aging; meta-analysis; metabolic syndrome; telomerase; telomere length
    DOI:  https://doi.org/10.3389/fgene.2024.1390198
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